Enantioselective Total Synthesis of Brevetoxin A: Unified Strategy for the B,E, G,and J Subunits |
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| Authors: | Michael T. Crimmins Prof. J. Michael Ellis Dr. Kyle A. Emmitte Dr. Pamela A. Haile Dr. Patrick J. McDougall Dr. Jonathan D. Parrish Dr. J. Lucas Zuccarello Dr. |
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| Affiliation: | Univeristy of North Carolina at Chapel Hill, Department of Chemistry, Chapel Hill, NC 27599‐3290 (USA), Fax: (+1) 919‐962‐2388 |
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| Abstract: | Brevetoxin A is a decacyclic ladder toxin that possesses 5‐, 6‐, 7‐, 8‐, and 9‐membered oxacycles, as well as 22 tetrahedral stereocenters. Herein, we describe a unified approach to the B, E, G, and J rings based upon a ring‐closing metathesis strategy from the corresponding dienes. The enolate technologies developed in our laboratory allowed access to the precursor acyclic dienes for the B, E, and G medium‐ring ethers. The strategies developed for the syntheses of these four monocycles ultimately provided multigram quantities of each of the rings, supporting our efforts toward the completion of a convergent synthesis of brevetoxin A. |
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| Keywords: | asymmetric synthesis chiral auxiliaries glycolate alkylation ring‐closing metathesis total synthesis |
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